Improved detection of cystic fibrosis mutations in infertility patients with DNA sequence analysis

doi:10.1093/humrep/deh134

Hum. Reprod. Advance Access published online on January 29, 2004
Human Reproduction, doi:10.1093/humrep/deh134
© 2004 by European Society of Human Reproduction and Embryology

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Received August 27, 2003
Accepted November 21, 2003

Article

Improved detection of cystic fibrosis mutations in infertility patients with DNA sequence analysis

Kari L. Danziger ¹, Lauri D. Black ², Steven B. Keiles ³, Anja Kammesheidt ³, and Paul J. Turek ⁴^*

¹ Department of Urology, University of California San Francisco, 1600 Divisadero Street, Box 1695, San Francisco, CA 94143-1695, USA
² Genetic Risk Assessment Program, California Pacific Medical Center, 3700 California St G330, San Francisco, CA 94118, USA
³ Ambry Genetics Corporation, 2060 Placentia Avenue, Suite A5, Costa Mesa, CA 92627, USA
⁴ Department of Urology, University of California San Francisco, 1600 Divisapturek@urol.ucsf.edudero Street, Box 1695, San Francisco, CA 94143-1695, USA

Abstract

BACKGROUND: Accurate determination of mutations in the cysticfibrosis transmembrane conductance regulator (CFTR) gene iscritical for genetic counselling and treatment of obstructiveazoospermia. Of concern is that detection rates with routineCFTR mutation panels vary widely depending on patient ancestry;and such panels have limited value for azoospermic patients,who are more likely to carry rare mutations. An alternativeapproach offers comprehensive, CFTR mutation analysis by a DNAsequence method. We investigated whether this method could improveCFTR detection rates in men with obstructive azoospermia ina prospective study of men with obstructive azoospermia andtheir partners who were referred for genetic counselling andtesting at one of two institutions. METHODS: Sixteen patientswith congenital absence of the vas deferens (CAVD, n = 14) oridiopathic obstructive azoospermia (n = 2) were studied. DNAfrom all patients was analysed for mutations by the DNA sequencemethod. In addition to this method, six men underwent CFTR analysisby a common 25 or 31 mutation panel coupled with poly T analysis.In 10 subjects, common mutation panel findings were inferredfrom DNA sequence method results. RESULTS: Overall, 12/16 (75%)azoospermic patients had one or more CFTR mutations and/or 5Talleles, including 12 mutations in 10 patients (two compoundheterozygotes) and seven 5T alleles in six patients (one homozygote).The sequence method detected all mutations and three variantsof unknown significance. By comparison, the common mutationpanels detected only 3/12 mutations (25%) and 0/3 variants.CONCLUSION: The DNA sequence method detects more CFTR mutationsthan common mutation panels. Given the serious, clinical consequencesof transmitting such mutations, this study underscores the importanceof accurate, CFTR mutation detection in men with obstructiveazoospermia and their partners.

Key words: Key words: azoospermia/congenital absence of the vas deferens/cystic fibrosis/genetic testing/male infertility

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